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RESULTS FROM THE 2005 ANNUAL REPORT

RESULTS FROM THE 2005 ANNUAL REPORT. SHOT - Organisation. SHOT was launched in 1996 A UK-wide confidential, voluntary anonymised scheme which aims to collect data on adverse events of transfusion of blood and blood components, and to make recommendations to improve transfusion safety

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RESULTS FROM THE 2005 ANNUAL REPORT

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  1. RESULTS FROM THE 2005 ANNUAL REPORT

  2. SHOT - Organisation • SHOT was launched in 1996 • A UK-wide confidential, voluntary anonymised scheme which aims to collect data on adverse events of transfusion of blood and blood components, and to make recommendations to improve transfusion safety • Based at Manchester Blood Centre

  3. SHOT - Organisation • Standing Working Group • Operational aspects Steering group • Strategic direction and “ownership” • Royal Colleges and professional bodies • Affiliated to the Royal College of Pathologists Funding • Four UK Blood Services on pro-rata basis according to the number of red cells issued

  4. SHOT - Aims • Through the participating Royal Colleges and professional bodies, SHOT findings can be used to: • inform policy within transfusion services • improve standards of hospital transfusion practice • aid production of clinical guidelines for the use of blood components • educate users on transfusion hazards and their prevention

  5. Categories of adverse events covered in the 2005 report • Incorrect blood/component transfused (IBCT) • Acute transfusion reaction (ATR) • Delayed transfusion reaction (DTR) • Transfusion-associated graft-versus-host-disease (TA-GvHD) • Transfusion-related acute lung injury (TRALI) • Post-transfusion purpura (PTP) • Transfusion transmitted infection, including bacterial contamination (TTI)

  6. Hospital participation - 2005 With the adoption of confidential ID numbers, SHOT is now able to provide every hospital with verification of participation. • 54%of eligible hospitals reported incidents in which a blood component was transfused. • 69%of eligible hospitals reported either at least one full incident or near miss.

  7. Numbers of incidents reported by individual hospitals 2005

  8. Breakdown of hospital reporting 2004 & 2005

  9. Summary of completed questionnaires (2005)

  10. Cumulative data 1996-2005

  11. Questionnaires analysed 1996 - 2005 (n=3239)

  12. Comparison of Report Types 1996 - 2005

  13. Cumulative mortality / morbidity table 1996-2005

  14. Cumulative mortality / morbidity according to the type of hazard reported 1996 – 2005 (1)

  15. Cumulative mortality / morbidity according to the type of hazard reported 1996 – 2005 (2)

  16. Major morbidity was defined as the presence of one or more of the following; • Intensive care admission and / or ventilation • Dialysis and / or renal impairment • Major haemorrhage from transfusion-induced coagulopathy • Intravascular haemolysis • Potential RhD sensitisation in a female of child-bearing potential

  17. Incorrect blood component transfused (IBCT) All reported episodes where a patient was transfused with a blood component or plasma product which did not meet the appropriate requirements or which was intended for another patient

  18. IBCT Cases reported 2005 524 completed questionnaires received Of these; 39 were withdrawn by the analyst (13 ‘right blood to right patient’ incidents, 26 did not meet IBCT criteria) 485 valid IBCT cases

  19. ABO incompatible red cell transfusions 1996 - 2005

  20. Mortality & morbidity - IBCT 2005 • 1 patient died following ABO incompatible red cell transfusion (imputability 3) • 1 patient died, possibly related to overtransfusion (imputability 1) • 1 patient suffered major morbidity due to overtransfusion (imputability 2) • 1 recipient of an ABO incompatible haemopoietic stem cell transplant received blood of the incorrect group and suffered a severe acute haemolytic reaction

  21. Cumulative mortality / morbidity data for IBCT cases 1996 - 2005(n=2317)

  22. Analysis of IBCT Cases

  23. 1. ‘Wrong Blood’ Events (n=87) • 10 patients received ABO incompatible red cell transfusions, 2 of which were also D incompatible. • 9 patients received ABO incompatibleFFP or cryoprecipitate (Group O components given to patients of other groups. • 2 patients received ABO incompatible platelets (Group O to patients of other groups in error) • 8 D negative patients received D positive cellular components - none was female of childbearing age. • 1 patient with anti-c received group O rr red cells. • 57 patients received components that were fortuitously compatible.

  24. ‘Wrong Blood’ Events - Site of Primary Error

  25. ‘Wrong Blood’ Events - Learning Points(1) • Basic training for biomedical scientists must reiterate careful sample identification at the point of test. • Robust systems must be in place for recording results of both manual and automated tests if electronic interfaces are not in place. • Competency based training for laboratory staff must include those working out of hours. • A laboratory quality system, as required by the Blood Safety & Quality Regulations, must include internal incident reporting mechanisms and appropriate, documented, corrective actions.

  26. ‘Wrong Blood’ Events - Learning Points(2) • A final patient identification check must always be carried out before transfusion using the identity band or formally risk assessed alternative attached to the patient. • Safety systems must be supported by training and education of all staff involved in transfusion, to ensure that correct procedures are followed. • Routine pre-transfusion testing should not be done outside of core hours unless there are adequate numbers of appropriately skilled staff.

  27. ‘Wrong Blood’ Events - Learning Points(3) • Administration of blood should only take place at night when clinically essential. • Procedures must be in place for collection of blood from refrigerators and must include the requirement to check against the patient’s minimum identification dataset.

  28. 2. Other Pre-transfusion Testing Errors (n=22) • 10 / 22 were errors involving the antibody screen. • 1 error involved a missed anti-A1. • 1 error where a repeat antibody panel was not done. • 2 cases where antigen negative units were not selected. • 1 case where electronic issue was used when an IAT crossmatch should have been performed. • 1 case where a laboratory failed to look for a masked allo-antibody in a patient with a positive DAT. • 5 cases where labs failed to request fresh samples for pre-transfusion testing from recently-transfused patients. • 1 case where a BMS entered negative results for a crossmatch that had not been performed.

  29. 3. Blood of wrong group given to recipients of ABO mismatched haemopoietic stem cell transplants (n=2) • In one case, the laboratory was not informed that the patient had received a transplant, and only suspected this when discrepant ABO grouping results started to develop. • In the second case the laboratory staff selected blood of the wrong group, then compounded the error by incorrectly performing the crossmatch and failing to detect incompatibility. The patient suffered an acute haemolytic reaction.

  30. 4. Failure to provide Components of appropriate specification or that did not meet special requirements (n=141)

  31. Failure to provide irradiated components (n=106)

  32. Site of primary error that led to failure to provide irradiated components

  33. Learning Points(1) • Hospital and laboratory IT systems should use compatible patient ID parameters to ensure that correct historical transfusion records are accessed rapidly and efficiently. Laboratory IT systems should be updated with special requirements and data should be transferred electronically to new systems. Systems should, if possible be updated with new rules eg MeBlue non-UK FFP for patients <16. • Several laboratory errors were caused by failure to notice the Special Requirements box on the transfusion request form. The format of transfusion request forms should be reviewed to ensure this section is appropriately prominent. Electronic requesting systems should ensure completion of this section is mandatory. Laboratories should also insist on appropriate clinical details on request forms.

  34. Learning Points(2) • Clinicians have a responsibility to be aware of the special transfusion needs of their patients and to ensure that local systems for notifying the laboratory are followed. Hospitals should consider implementing a system of informing the laboratory as soon as transfusion for irradiated components is identified. In the case of purine analogue therapy, routine notification of the transfusion laboratory by the hospital pharmacy is an effective safety measure, although data should be transferred at frequent intervals to prevent patients receiving non-irradiated products in the ‘window period’. Where patients have several volumes of hospital notes, each should be ‘flagged’ with the special requirements.

  35. Learning Points(3) • Blood request forms must be accurately completed and transfusion prescriptions must indicate special requirements. • The final bedside check is the last barrier to mistransfusion and appears to fail in 20 - 40% of cases - research into ways of improving its effectiveness and evaluation of new technologies to improve the process is essential. • Communication both between clinicians in specialist treatment centres and local hospitals, and between clinical teams within hospitals, must be improved. Data on special transfusion requirements should be communicated between transfusion laboratories in hospitals that routinely ‘share’ patients.

  36. Learning Points(4) • Greater emphasis should be placed on involving patients in ensuring their special transfusion requirements are met. Simply issuing ‘Irradiated Component’ cards to patients appears to have been of limited benefit. The introduction of a patient held booklet (analogous to the commonly used anticoagulant booklet), together with targeted education, should be considered for patients following stem cell transplantation and purine analogue therapy and would be a suitable area for clinical research and pilot studies.

  37. 5. Inappropriate or unnecessary transfusions (n=67)

  38. Learning Points • All staff undertaking phlebotomy must understand the importance of correct patient identification and correct sampling technique, and must be assessed as competent. • Blood should only be prescribed by a doctor who has undergone training in blood transfusion and been assessed as competent. • Diagnostic laboratories must carry out checks to identify large changes in parameters (‘delta checks’) and should communicate discrepancies to other laboratories. • Near patient testing must be subject to the same standards of validation and quality assurance as the diagnostic laboratory.

  39. 6. ‘Unsafe’ transfusions (n=79)

  40. Learning Points(1) • The need for every satellite refrigerator should be carefully risk assessed and reviewed regularly. Clear protocols establishing the responsibilities of the laboratory and nursing staff must be implemented. • Transfusion laboratory stock control procedures should ensure that expired units are cleared from issue locations. • Nurses giving blood must be familiar with current guidelines on the handling of blood components.

  41. Learning Points(2) • Competency training for ward staff must reiterate the requirement for red cells to ONLY be stored in monitored blood refrigerators and must highlight the differences between a blood refrigerator and a normal ward refrigerator. • Pre-transfusion checking procedures must include checking of the expiry date of the component and noting any end-date for suitability provided by the laboratory.

  42. 7. Adverse events relating to anti-D immunoglobulin (Ig) (n=87)

  43. Learning Points • Training and competency assessment of BMSs in antenatal serology testing and the indications for issue of anti-D Ig must be comprehensive. • There is an urgent need for education of primary care staff in the basic principles of antenatal serology and current relevant guidelines.

  44. Summary of blood transfusion laboratory errors - all cases (where known)

  45. ‘Right blood to right patient’ - RBRP (n=67)

  46. RBRP - the checking procedures that failed to identify the error(s)

  47. Learning Points • Clinicians should be aware of the potential dangers of transfusing patients when the checking process has highlighted a discrepancy in available information. If the situation is not an emergency it must be standard policy not to transfuse and to begin the process again. • Staff carrying out the bedside check must check all details in minute detail since a discrepancy in only one letter or digit is potentially dangerous.

  48. Near Miss Events Any error which, if undetected, could result in the determination of a wrong blood group, or issue, collection or administration of an incorrect, inappropriate or unsuitable component, but which was recognised before transfusion took place

  49. Near Miss Events

  50. Types of “Near miss” events • Sample errors (806) • Request errors (145) • Laboratory sample handling &/or testing errors (87) • Laboratory component selection, handling, storage & issue errors (111) • Component collection, transportation, ward handling & administrationerrors (209)

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